A novel role for nucleolin in splice site selection

Shefer, Kinneret; Boulos, Ayub; Gotea, Valer; Arafat, Maram; Chaim, Yair Ben; Muharram, Aya; Isaac, Sara; Eden, Amir; Sperling, Joseph; Elnitski, Laura; Sperling, Ruth

doi:10.1080/15476286.2021.2020455

Cited by 6 publications

(2 citation statements)

References 87 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Finally, NCL knockdown resulted in activation of latent splicing in hundreds of coding transcripts that have important cellular functions. We thus proposed NCL as the first protein component in a nuclear quality control mechanism that regulates splice site selection, thereby protecting cells from latent splicing that can generate defective mRNAs [ 46 ].…”

Section: Elements Of the Sos Mechanismmentioning

confidence: 99%

“…We propose that, at this stage, NCL can now be added in the model as a protein directly binding ini-tRNA, likely along with additional proteins. This step helps establish a register for the recognition of the reading frame [ 46 ]. The second SOS element involves the cooperative polymerization of protein(s) that bind triplets of nucleotides and in the absence of a PTC it reaches the selected 5′SS; this step is the quality control “confirmation” step of SS selection that triggers the remodeling of the spliceosome to its functional state ( Figure 3 b, left).…”

Section: An Updated Model Of the Sos Mechanismmentioning

confidence: 99%

See 1 more Smart Citation

A Quality Control Mechanism of Splice Site Selection Abrogated under Stress and in Cancer

Arafat

Sperling

2022

Cancers

Self Cite

View full text Add to dashboard Cite

Latent 5’ splice sites, highly abundant in human introns, are not normally used. This led to the proposal of a quality control mechanism, Suppression of Splicing (SOS), which protects cells from splicing at the numerous intronic latent sites, and whose activation can generate nonsense mRNAs. SOS was shown to be independent of Nonsense-Mediated mRNA Decay (NMD). Efforts to decipher the SOS mechanism revealed a pivotal role for initiator-tRNA, independent of protein translation. Recently, nucleolin (a multifunctional protein) was found to directly and specifically bind the initiator-tRNA in the nucleus and was shown to be a protein component of SOS, enabling an updated model of the SOS mechanism. Importantly, SOS is abrogated under stress and in cancer (e.g., in breast cancer cells and gliomas), generating thousands of nonsense mRNAs due to activation of latent splicing. The resulting affected human genes cover a variety of functional groups, including genes involved in cell proliferation and differentiation. Furthermore, in oligodendroglioma, the extent of activation of latent splicing increases with the severity of the cancer. Interesting examples are genes expressing aberrant nonsense mRNAs in both breast cancer and glioma, due to latent splicing activation. These findings highlight the unexplored potential of such aberrant isoforms as novel targets for cancer diagnosis and therapies.

show abstract

Section: Elements Of the Sos Mechanismmentioning

confidence: 99%

Section: An Updated Model Of the Sos Mechanismmentioning

confidence: 99%